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Data from Arginase 1/2 Inhibitor OATD-02: From Discovery to First-in-man Setup in Cancer Immunotherapy

Posted on 2023-07-05 - 08:21
Abstract

Pharmacologic inhibition of the controlling immunity pathway enzymes arginases 1 and 2 (ARG1 and ARG2) is a promising strategy for cancer immunotherapy. Here, we report the discovery and development of OATD-02, an orally bioavailable, potent arginases inhibitor. The unique pharmacologic properties of OATD-02 are evidenced by targeting intracellular ARG1 and ARG2, as well as long drug-target residence time, moderate to high volume of distribution, and low clearance, which may jointly provide a weapon against arginase-related tumor immunosuppression and ARG2-dependent tumor cell growth. OATD-02 monotherapy had an antitumor effect in multiple tumor models and enhanced an efficacy of the other immunomodulators. Completed nonclinical studies and human pharmacokinetic predictions indicate a feasible therapeutic window and allow for proposing a dose range for the first-in-human clinical study in patients with cancer.

Significance:

We have developed an orally available, small-molecule intracellular arginase 1 and 2 inhibitor as a potential enhancer in cancer immunotherapy. Because of its favorable pharmacologic properties shown in nonclinical studies, OATD-02 abolishes tumor immunosuppression induced by both arginases, making it a promising drug candidate entering clinical trials.

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FUNDING

European Regional Development Fund (ERDF)

Narodowe Centrum BadaƄ i Rozwoju (NCBR)

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Molecular Cancer Therapeutics

AUTHORS (40)

  • Bartlomiej Borek
    Julita Nowicka
    Anna Gzik
    Marek Dziegielewski
    Karol Jedrzejczak
    Joanna Brzezinska
    Marcin Grzybowski
    Paulina Stanczak
    Paulina Pomper
    Agnieszka Zagozdzon
    Tomasz Rejczak
    Krzysztof Matyszewski
    Adam Golebiowski
    Jacek Olczak
    Kamil Lisiecki
    Magdalena Tyszkiewicz
    Magdalena Kania
    Sylwia Piasecka
    Anna Cabaj
    Paulina Dera

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